Id-1, Id-2, and Id-3 co-expression correlates with prognosis in stage I and II lung adenocarcinoma patients treated with surgery and adjuvant chemotherapy.
Antonângelo. Leila L; Tuma. Taila T; Fabro. Alexandre A; Acencio. Milena M; Terra. Ricardo R; Parra. Edwin E; Vargas. Francisco F; Takagaki. Teresa T; Capelozzi. Vera V
Key Findings
- Id‑1, Id‑2, and Id‑3 are expressed at higher levels in lung adenocarcinoma tumors than in normal lung tissue.
- High nuclear Id‑1 is associated with increased blood vessel growth (angiogenesis) in the tumor.
- High cytoplasmic Id‑3 correlates with lymph‑node metastasis and shorter metastasis‑free survival.
- Both high Id‑1 and Id‑3 levels predict a higher risk of death, independent of cancer stage.
Practical Outcomes
- The findings are specific to lung cancer prognosis and do not translate into actionable steps for longevity, metabolic health, or performance enhancement. There are no recommended supplements, dosages, or lifestyle changes derived from this research for the biohacker community.
Summary
This study looked at three proteins (Id‑1, Id‑2, Id‑3) in lung cancer tissue and found that higher levels of Id‑1 and Id‑3 are linked to worse survival and more aggressive disease, but it doesn’t give any advice you can use for everyday health or performance.
Abstract
Inhibitors of DNA binding/inhibitors of differentiation (Id) protein family have been shown to be involved in carcinogenesis. However, the roles of Id during lung adenocarcinoma (ADC) progression remain unclear. Eighty-eight ADC samples were evaluated for Id-1,2,3 level and angiogenesis (CD 34 and VEGF microvessel density) by immunohistochemistry and morphometry. The impact of these markers was tested on follow-up until death or recurrence. A significant difference between tumor and normal tissue was found for Id-1,2,3 expression (P < 0.01). In addition, high levels of nuclear Id-1 were associated with higher angiogenesis in the tumor stroma (P < 0.01). Equally significant was the association between patients in T1-stage and low cytoplasmic Id-2, as well as patients in stage-IIb and low Id-3. High cytoplasm Id-3 expression was also directly associated to lymph nodes metastasis (P = 0.05). Patients at stages I to III, with low Id-1 and Id-3 cytoplasm histoscores showed significant long metastasis-free survival time than those with high Id-1 or Id-3 expression (P = 0.04). Furthermore, high MVD-CD34 and MVD-VEGF expression were associated with short recurrence-free survival compared to low MVD-CD34 and MVD-VEGF expressions (P = 0.04). Cox model analyses controlled for age, lymph node metastasis, and adjuvant treatments showed that nuclear Id-1, cytoplasmic Id-3, and MVD-CD34 were significantly associated with survival time. Median score for nuclear Id-1 and cytoplasmic Id-3 divided patients in two groups, being that those with increased Id-1 and Id-3 presented higher risk of death. Ids showed an independent prognostic value in patients with lung ADC, regardless of disease stage. Id-1 and Id-3 should be considered new target candidates in the development of personalized therapy in lung ADC.
Study Information
pubmed
2016
2016-02-10T00:00:00.000Z
10.1177/1535370216632623
13
46